在明显的弥散性血管内凝血中补充抗凝血酶 III 的临床结果:单一机构的纵向经验和回顾性分析。

4区 医学 Q2 Nursing
Annals of palliative medicine Pub Date : 2024-05-01 Epub Date: 2024-04-23 DOI:10.21037/apm-23-535
SongAm Lee, JunSeok Kim, Michael Ji, HyeongJu Moon, WooSurng Lee
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引用次数: 0

摘要

背景:抗凝血酶是一种在肝脏合成的小型血浆糖蛋白,属于丝氨酸蛋白酶抑制剂的丝氨酸蛋白家族,能使凝血途径中的几种酶失活。它在凝血途径中起着主导作用,因此,抗凝血酶是治疗弥散性血管内凝血(DIC)等严重临床疾病的必要药物。尽管理论上补充抗凝血酶有好处,但肝素疗效的最佳抗凝血酶活性以及在各种疾病中补充抗凝血酶的好处尚未完全清楚:国家医疗保险局和食品药品安全部对 DIC 病例中抗凝血酶 III 的严格管理准则如下:成人抗凝血酶水平低于 20 mg/dL;成人抗凝血酶活性低于正常水平的 70%;抗凝血酶的总用药时间必须严格限制在最长 3 天内,总用药剂量必须低于 7000 国际单位(IU)(负荷剂量,1 小时内 1000 IU;维持剂量,每 6 小时 500 IU,持续 3 天):根据上述标准,我们在本机构确定了 76 名符合分析条件的患者(男/女,59/17)。其中 44 名患者被认定为非存活组,32 名患者被认定为存活组。非存活组和存活组的基线参数相当,在年龄(66.5±18.1 岁 vs. 66.0±16.2岁,P=0.90)、性别(32/12 vs. 27/5,P=0.35)、住院时间(31.1±34.5 天 vs. 31.2±26.1 天,P=0.99)、器官功能衰竭序列评估(SOFA)(7.3±2.5 vs. 6.6±2.0,P=0.22)、简化急性生理学评分 II(SAPS II)(46.0±8.8 vs. 43.5±9.2,P=0.23)、DIC 原因(P=0.95)和基础疾病(P=0.38)。非存活组在用药前一天的抗凝血酶 III 水平明显低于存活组(50.1%±13.6% vs. 57.6%±12.5%,P=0.01)。服用抗凝血酶 III 后第 2 天和第 7 天的血红蛋白水平在非幸存者组和幸存者组之间存在显著差异(9.9±1.9 vs. 11.0±2.0 g/dL,P=0.01;9.4±1.8 vs. 10.5±1.6 g/dL,P=0.006)。用药当天的抗凝血酶 III 水平[曲线下面积(AUC)=0.672]比第 1 天(AUC=0.552)、第 2 天(AUC=0.624)和第 7 天(AUC=0.593)的抗凝血酶 III 水平对死亡率的预测效果明显更好:我们的研究表明,服用抗凝血酶可能是治疗 DIC 的有效手段,尤其是在 DIC 的病例中,可以给予更积极的考虑,因为 DIC 是脓毒性休克、脓毒症和其他危重疾病的常见并发症,死亡率很高。此外,我们的研究还表明,国家指南推荐的抗凝血酶给药总剂量和给药时间可能不够,因此可能有必要延长给药时间和增加抗凝血酶补充剂的总剂量。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Clinical outcomes of antithrombin III supplementation in an overt disseminated intravascular coagulation: a longitudinal single-institutional experience and retrospective analysis.

Background: Antithrombin is a small plasma glycoprotein synthesized in the liver that belongs to the serpin family of serine protease inhibitors and inactivates several enzymes in the coagulation pathway. It plays a leading major factor on coagulation pathway, therefore administration of antithrombin is essential to treat serious clinical conditions such as disseminated intravascular coagulation (DIC). Despite the theoretical benefits of antithrombin supplementation, the optimal antithrombin activity for heparin efficacy and the benefits of antithrombin supplementation in various disease entities are not yet fully understood.

Methods: The strict administration guidelines on antithrombin III in cases of DIC by the National Health Insurance Service and the Ministry of Food and Drug Safety complied as follows: antithrombin levels below 20 mg/dL in adults; antithrombin activity below 70% of normal in adults; total administration period of antithrombin must be carefully limited to within maximum 3 days, and the total administration dose must be below 7,000 international unit (IU), (loading dose, 1,000 IU in 1 hour: maintenance dose, 500 IU every 6 hours for 3 days).

Results: We identified 76 eligible for analysis according to the above-mentioned criteria in our institution (male/female, 59/17). Forty-four were identified to the non-survivor group and 32 patients were recognized as the survivor group. The baseline parameters in the non-survivor and survivor groups were comparable with no significant differences in age (66.5±18.1 vs. 66.0±16.2 years, P=0.90), sex (32/12 vs. 27/5, P=0.35), hospital length of stay (31.1±34.5 vs. 31.2±26.1 days, P=0.99), sequential organ failure assessment (SOFA) (7.3±2.5 vs. 6.6±2.0, P=0.22), simplified acute physiology score II (SAPS II) (46.0±8.8 vs. 43.5±9.2, P=0.23), cause for DIC (P=0.95), and underlying disease (P=0.38). The levels of antithrombin III on the day just before the administration significantly lower in the non-survivor groups than in the survivor groups (50.1%±13.6% vs. 57.6%±12.5%, P=0.01). The hemoglobin level in the 2nd day and 7th day after antithrombin III administration was significantly different between the non-survivor and survivor groups (9.9±1.9 vs. 11.0±2.0 g/dL, P=0.01, and 9.4±1.8 vs. 10.5±1.6 g/dL, P=0.006). The antithrombin III levels on the day of administration [area under the curve (AUC) =0.672] demonstrated significantly better prediction of mortality than the A antithrombin III levels on 1st day (AUC =0.552), the 2nd day (AUC =0.624), and 7th day (AUC =0.593).

Conclusions: Our study suggests that the antithrombin administration may be effective tools for DIC treatment, and may be more positively considered, especially in the cases of DIC, which is a frequent complication of septic shock, sepsis, and other critical disease entities and which is associated with a high level of mortality. Furthermore, our study also suggests that the total doses and periods of antithrombin administration, which recommended by national guidelines, may be insufficient, therefore prolongation of period and increase of total dose of antithrombin supplement might be necessary.

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来源期刊
Annals of palliative medicine
Annals of palliative medicine Medicine-Anesthesiology and Pain Medicine
自引率
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231
期刊介绍: Annals of Palliative Medicine (Ann Palliat Med; Print ISSN 2224-5820; Online ISSN 2224-5839) is an open access, international, peer-reviewed journal published quarterly with both online and printed copies since 2012. The aim of the journal is to provide up-to-date and cutting-edge information and professional support for health care providers in palliative medicine disciplines to improve the quality of life for patients and their families and caregivers.
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